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Association of P2Y12 Gene Promoter DNA Methylation with the Risk of Clopidogrel Resistance in Coronary Artery Disease Patients

机译:P2Y12基因启动子DNA甲基化与冠心病患者氯吡格雷抵抗风险的关系

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Background. Clopidogrel inhibits the ADP receptor P2Y12 to keep down the platelet aggregation. The goal of our study is to investigate the contribution of P2Y12 promoter DNA methylation to the risk of clopidogrel resistance (CR). Methods. The platelet functions were measured by the VerifyNow P2Y12 assay. Applying the bisulfite pyrosequencing technology, DNA methylation levels of two CpG dinucleotides on P2Y12 promoter were tested among 49 CR cases and 57 non-CR controls. We also investigated the association among P2Y12 DNA methylation, various biochemical characteristics, and CR. Result. Lower methylation of two CpGs indicated the poorer clopidogrel response (CpG1, P = 0.009; CpG2, P = 0.022) in alcohol abusing status. Meanwhile CpG1 methylation was inversely correlated with CR in smoking patients (P = 0.026) and in subgroup of Albumin < 35 (P = 0.002). We observed that the level of DNA methylation might be affected by some clinical markers, such as TBIL, LEVF, Albumin, AST. The results also showed that the quantity of stent, fasting blood-glucose, and lower HbACl were the predictors of CR. Conclusions. The evidence from our study indicates that P2Y12 methylation may bring new hints to elaborate the pathogenesis of CR.
机译:背景。氯吡格雷可抑制ADP受体P2Y12抑制血小板聚集。我们研究的目的是研究P2Y12启动子DNA甲基化对氯吡格雷抵抗(CR)风险的影响。方法。通过VerifyNow P2Y12测定法测量血小板功能。应用亚硫酸氢盐焦磷酸测序技术,在49例CR病例和57例非CR对照中检测了P2Y12启动子上两个CpG二核苷酸的DNA甲基化水平。我们还调查了P2Y12 DNA甲基化,各种生化特征和CR之间的关联。结果。在酒精滥用状态下,两个CpG的甲基化程度较低表明氯吡格雷反应较差(CpG1,P = 0.009; CpG2,P = 0.022)。同时,吸烟患者和白蛋白<35的亚组中CpG1甲基化与CR呈负相关(P = 0.002)。我们观察到DNA甲基化的水平可能受某些临床标志物的影响,例如TBIL,LEVF,白蛋白,AST。结果还表明,支架数量,空腹血糖和较低的HbACl是CR的预测指标。结论我们研究的证据表明,P2Y12甲基化可能为阐明CR的发病机理带来新的提示。

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